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固有和适应性白细胞介素 17 产生细胞在慢性炎症性肺部疾病中的作用。

Innate and adaptive interleukin-17-producing lymphocytes in chronic inflammatory lung disorders.

机构信息

Katholieke Universiteit Leuven, Laboratory of Pneumology, Lung Transplantation Unit, 49 Herestraat, Leuven, Belgium.

出版信息

Am J Respir Crit Care Med. 2011 Apr 15;183(8):977-86. doi: 10.1164/rccm.201007-1196PP. Epub 2010 Nov 19.

DOI:10.1164/rccm.201007-1196PP
PMID:21097694
Abstract

During T-cell receptor activation in a particular cytokine environment, naive CD4+ T cells may differentiate into lineages defined by their pattern of cytokine production and transcription factors: T helper type 1 (Th1), Th2, Th17, and Th22 cells; follicular helper T cells; and inducible regulatory T cells. Th17 cells have been recognized as a distinct lineage of Th cells, and associations between IL-17 and human disease have been known somewhat longer. It would be an oversimplification to restrict IL-17 to Th17 cells. Indeed, IL-17 is also expressed by other cells including IL-17-producing γδ T (γδ T-17) cells, natural killer T-17 cells, and IL-17-producing lymphoid tissue-induced cells. IL-17 was cloned in 1995 as a cytokine expressed by T cells, exerting inflammatory effects on epithelial, endothelial, and fibroblast cells. IL-17 is a solid link between innate and adaptive immunity and can exert both beneficial and deleterious effects. The discovery of IL-17 T cells has provided exciting new insights into host defense, immunoregulation, and autoimmunity. Unquestionably, data from mouse models have contributed enormously to our insight into immunological mechanisms. However, because of numerous differences between murine and human immunology, data obtained in mice are not simply interchangeable. We review IL-17 T cells exclusively in the human situation and more specifically their potential role in respiratory diseases. The advances in our understanding of IL-17 regulation offer opportunities to dissect the human IL-17 system and to reflect on the clinical presentation of lung diseases. More importantly, the IL-17 system allows us to speculate on new therapeutic opportunities. Some results have been previously reported in an abstract.

摘要

在特定细胞因子环境下 T 细胞受体激活时,初始 CD4+T 细胞可能会根据其细胞因子产生和转录因子的模式分化为不同谱系:辅助性 T 细胞 1(Th1)、Th2、Th17 和 Th22 细胞;滤泡辅助 T 细胞;诱导性调节性 T 细胞。Th17 细胞已被认为是辅助性 T 细胞的一个独特谱系,而 IL-17 与人类疾病之间的关联也已为人所知一段时间了。将 IL-17 仅限于 Th17 细胞是过于简单化的。事实上,IL-17 也由其他细胞表达,包括产生 IL-17 的 γδ T(γδ T-17)细胞、自然杀伤 T-17 细胞和产生 IL-17 的淋巴组织诱导细胞。1995 年,IL-17 作为一种由 T 细胞表达的细胞因子被克隆,对上皮细胞、内皮细胞和成纤维细胞发挥炎症作用。IL-17 是先天免疫和适应性免疫之间的牢固联系,可以发挥有益和有害的作用。IL-17 T 细胞的发现为宿主防御、免疫调节和自身免疫提供了令人兴奋的新见解。毫无疑问,来自小鼠模型的数据极大地促进了我们对免疫机制的理解。然而,由于鼠类和人类免疫学之间存在许多差异,在小鼠中获得的数据不能简单地互换。我们仅在人类情况下综述 IL-17 T 细胞,更具体地说,它们在呼吸疾病中的潜在作用。我们对 IL-17 调节的理解的进展为剖析人类 IL-17 系统和反思肺部疾病的临床表现提供了机会。更重要的是,IL-17 系统使我们能够推测出新的治疗机会。一些结果以前曾在摘要中报道过。

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